Date published: 2025-9-17

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WFDC1B Activators

Chemical activators of WFDC1B can trigger its activation through various biochemical pathways that involve modulation of intracellular signaling cascades. Forskolin, for instance, directly stimulates adenylate cyclase, thereby increasing the levels of cyclic AMP (cAMP) within the cell. This rise in cAMP activates protein kinase A (PKA), which can then phosphorylate WFDC1B, leading to its activation. Similarly, Dibutyryl cAMP, a synthetic analog of cAMP, bypasses the need for adenylate cyclase stimulation and directly activates PKA, subsequently promoting the activation of WFDC1B. Another activator, Phorbol 12-myristate 13-acetate (PMA), is a potent activator of protein kinase C (PKC), which phosphorylates target proteins like WFDC1B, thereby enhancing its activity.

On the other hand, ionomycin functions by increasing the intracellular concentration of calcium, which activates calmodulin-dependent kinases capable of phosphorylating WFDC1B. Similarly, calcium chloride also raises intracellular calcium levels, leading to the activation of kinases that can directly phosphorylate and activate WFDC1B. Magnesium chloride can enhance the activity of these kinases further. In a different mechanism, Zinc acetate may activate WFDC1B by stabilizing its structure through binding to zinc-binding domains within the protein, or even directly triggering an activation conformation. Reactive oxygen species such as hydrogen peroxide can initiate cellular pathways that lead to the activation of WFDC1B, though the exact mechanism may involve several steps, including kinase activation. Sodium fluoride acts by inhibiting phosphatases, which normally dephosphorylate and deactivate WFDC1B, thus maintaining WFDC1B in a phosphorylated, active state. In a similar vein, okadaic acid inhibits phosphatases leading to sustained phosphorylation and activation of WFDC1B. Lastly, compounds like anisomycin and thapsigargin activate stress-activated protein kinases and disrupt calcium homeostasis, respectively, both of which can lead to the phosphorylation and activation of WFDC1B through upstream signaling events.

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